EBioMedicine (Sep 2023)

Transient anti-cytokine autoantibodies superimpose the hyperinflammatory response in Kawasaki disease and multisystem inflammatory syndrome in children: a comparative cohort study on correlates of diseaseResearch in context

  • Stejara A. Netea,
  • Giske Biesbroek,
  • Diana van Stijn,
  • Hanna Ijspeert,
  • Caspar I. van der Made,
  • Machiel H. Jansen,
  • Judy Geissler,
  • J.M. (Merlijn) van den Berg,
  • Martijn van der Kuip,
  • Mariken P. Gruppen,
  • Dieneke Schonenberg-Meinema,
  • Berber Kapitein,
  • A.M. (Marceline) Tutu van Furth,
  • Sietse Q. Nagelkerke,
  • Dasja Pajkrt,
  • Frans B. Plötz,
  • M.E.J. (Lisette) den Boer,
  • Gijs W. Landman,
  • Marlies A. van Houten,
  • Ines Goetschalckx,
  • Erik J.M. Toonen,
  • Frank L. van de Veerdonk,
  • Irene M. Kuipers,
  • Willem A. Dik,
  • Taco W. Kuijpers,
  • T. Hendriks,
  • M.K. Felderhof,
  • N.M. Weggelaar,
  • L. Filippini,
  • L. Rozendaal,
  • M. Groeneweg,
  • R. Nuboer,
  • M. Bruijn,
  • K.M. Dolman,
  • J.G. Noordzij,
  • J.P. de Winter,
  • A.M. Vlieger,
  • F.B. Plötz,
  • L.C. Delemarre

Journal volume & issue
Vol. 95
p. 104736

Abstract

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Summary: Background: Children with SARS-CoV-2 related Multisystem Inflammatory Syndrome in Children (MIS-C) often present with clinical features that resemble Kawasaki disease (KD). Disease severity in adult COVID-19 is associated to the presence of anti-cytokine autoantibodies (ACAAs) against type I interferons. Similarly, ACAAs may be implicated in KD and MIS-C. Therefore, we explored the immunological response, presence of ACAAs and disease correlates in both disorders. Methods: Eighteen inflammatory plasma protein levels and seven ACAAs were measured in KD (n = 216) and MIS-C (n = 56) longitudinally by Luminex and/or ELISA. Levels (up to 1 year post-onset) of these proteins were related to clinical data and compared with healthy paediatric controls. Findings: ACAAs were found in both patient groups. The presence of ACAAs lagged behind the inflammatory plasma proteins and peaked in the subacute phase. ACAAs were mostly directed against IFN-γ (>80%) and were partially neutralising at best. KD presented with a higher variety of ACAAs than MIS-C. Increased levels of anti-IL-17A (P = 0·02) and anti-IL-22 (P = 0·01) were inversely associated with ICU admission in MIS-C. Except for CXCL10 in MIS-C (P = 0·002), inflammatory plasma proteins were elevated in both KD and MIS-C. Endothelial angiopoietin-2 levels were associated with coronary artery aneurysms in KD (P = 0·02); and sCD25 (P = 0·009), angiopoietin-2 (P = 0·001), soluble IL-33-receptor (ST2, P = 0·01) and CXCL10 (P = 0·02) with ICU admission in MIS-C. Interpretation: Markers of endothelial activation (E-selectin, angiopoietin-2), and innate and adaptive immune responses (macrophages [CD163, G-CSF], neutrophils [lipocalin-2], and T cells [IFN-γ, CXCL10, IL-6, IL-17]), are upregulated in KD and MIS-C. ACAAs were detected in both diseases and, although only partly neutralising, their transient presence and increased levels in non-ICU patients may suggest a dampening role on inflammation. Funding: The Kawasaki study is funded by the Dutch foundation Fonds Kind & Handicap and an anonymous donor. The sponsors had no role in the study design, analysis, or decision for publication.

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